| Literature DB >> 36090450 |
Xingcheng Lin1,2,3, Jason T George1,4, Nicholas P Schafer1,5, Kevin Ng Chau6, Michael E Birnbaum7,8,9, Cecilia Clementi1,5,10, José N Onuchic1,2,5,11, Herbert Levine1,6.
Abstract
Accurate assessment of TCR-antigen specificity at the whole immune repertoire level lies at the heart of improved cancer immunotherapy, but predictive models capable of high-throughput assessment of TCR-peptide pairs are lacking. Recent advances in deep sequencing and crystallography have enriched the data available for studying TCR-p-MHC systems. Here, we introduce a pairwise energy model, RACER, for rapid assessment of TCR-peptide affinity at the immune repertoire level. RACER applies supervised machine learning to efficiently and accurately resolve strong TCR-peptide binding pairs from weak ones. The trained parameters further enable a physical interpretation of interacting patterns encoded in each specific TCR-p-MHC system. When applied to simulate thymic selection of an MHC-restricted T-cell repertoire, RACER accurately estimates recognition rates for tumor-associated neoantigens and foreign peptides, thus demonstrating its utility in helping address the large computational challenge of reliably identifying the properties of tumor antigen-specific T-cells at the level of an individual patient's immune repertoire.Entities:
Year: 2021 PMID: 36090450 PMCID: PMC9455901 DOI: 10.1038/s43588-021-00076-1
Source DB: PubMed Journal: Nat Comput Sci ISSN: 2662-8457